Recurrent heterozygous PAX6 missense variants cause severe bilateral microphthalmia via predictable effects on DNA-protein interaction

Kathleen Williamson; H. Nikki Hall; Liusaidh Owen; Benjamin Livesey; Isabel Hanson; G.G.W Adams; Simon Bodek; Patrick Calvas; Bruce Castle; Michael Clarke; Alexander T Deng; Patrick Edery; Richard Fisher; Gabriele Gillessen-Kaesbach; Elise Héon; Jane Hurst; Dragana Josifova; Birgit Lorenz; Shane McKee; Francoise Meire; Anthony T Moore; Michael Parker; Charlotte Reiff; Jay Self; Edward S Tobias; Joke B. G. M. Verheij; Marjolaine Willems; Denise Williams; Veronica Van Heyningen; Joseph A. Marsh; David R. FitzPatrick

doi:10.1038/s41436-019-0685-9

Recurrent heterozygous PAX6 missense variants cause severe bilateral microphthalmia via predictable effects on DNA-protein interaction

Kathleen Williamson, H. Nikki Hall, Liusaidh Owen, Benjamin Livesey, Isabel Hanson, G.G.W Adams, Simon Bodek, Patrick Calvas, Bruce Castle, Michael Clarke, Alexander T Deng, Patrick Edery, Richard Fisher, Gabriele Gillessen-Kaesbach, Elise Héon, Jane Hurst, Dragana Josifova, Birgit Lorenz, Shane McKee, Francoise MeireAnthony T Moore, Michael Parker, Charlotte Reiff, Jay Self, Edward S Tobias, Joke B. G. M. Verheij, Marjolaine Willems, Denise Williams, Veronica Van Heyningen, Joseph A. Marsh, David R. FitzPatrick

Research output: Contribution to journal › Article › peer-review

Abstract

Purpose
Most classical aniridia is caused by PAX6 haploinsufficiency. PAX6 missense variants can be hypomorphic or mimic haploinsufficiency. We hypothesized that missense variants also cause previously undescribed disease by altering the affinity and/or specificity of PAX6 genomic interactions.

Methods
We screened PAX6 in 372 individuals with bilateral microphthalmia, anophthalmia, or coloboma (MAC) from the Medical Research Council Human Genetics Unit eye malformation cohort (HGUeye) and reviewed data from the Deciphering Developmental Disorders study. We performed cluster analysis on PAX6-associated ocular phenotypes by variant type and molecular modeling of the structural impact of 86 different PAX6 causative missense variants.

Results
Eight different PAX6 missense variants were identified in 17 individuals (15 families) with MAC, accounting for 4% (15/372) of our cohort. Seven altered the paired domain (p.[Arg26Gln]x1, p.[Gly36Val]x1, p.[Arg38Trp]x2, p.[Arg38Gln]x1, p.[Gly51Arg]x2, p.[Ser54Arg]x2, p.[Asn124Lys]x5) and one the homeodomain (p.[Asn260Tyr]x1). p.Ser54Arg and p.Asn124Lys were exclusively associated with severe bilateral microphthalmia. MAC-associated variants were predicted to alter but not ablate DNA interaction, consistent with the electrophoretic mobility shifts observed using mutant paired domains with well-characterized PAX6-binding sites. We found no strong evidence for novel PAX6-associated extraocular disease.

Conclusion
Altering the affinity and specificity of PAX6-binding genome-wide provides a plausible mechanism for the worse-than-null effects of MAC-associated missense variants.

Original language	English
Journal	Genetics in Medicine
DOIs	https://doi.org/10.1038/s41436-019-0685-9
Publication status	Published - 8 Nov 2019

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Williamson, K., Hall, H. N., Owen, L., Livesey, B., Hanson, I., Adams, G. G. W., Bodek, S., Calvas, P., Castle, B., Clarke, M., Deng, A. T., Edery, P., Fisher, R., Gillessen-Kaesbach, G., Héon, E., Hurst, J., Josifova, D., Lorenz, B., McKee, S., ... FitzPatrick, D. R. (2019). Recurrent heterozygous PAX6 missense variants cause severe bilateral microphthalmia via predictable effects on DNA-protein interaction. Genetics in Medicine. https://doi.org/10.1038/s41436-019-0685-9

@article{13fdec9fb39c432787e1e8526d8c1c5f,

title = "Recurrent heterozygous PAX6 missense variants cause severe bilateral microphthalmia via predictable effects on DNA-protein interaction",

abstract = "PurposeMost classical aniridia is caused by PAX6 haploinsufficiency. PAX6 missense variants can be hypomorphic or mimic haploinsufficiency. We hypothesized that missense variants also cause previously undescribed disease by altering the affinity and/or specificity of PAX6 genomic interactions.MethodsWe screened PAX6 in 372 individuals with bilateral microphthalmia, anophthalmia, or coloboma (MAC) from the Medical Research Council Human Genetics Unit eye malformation cohort (HGUeye) and reviewed data from the Deciphering Developmental Disorders study. We performed cluster analysis on PAX6-associated ocular phenotypes by variant type and molecular modeling of the structural impact of 86 different PAX6 causative missense variants.ResultsEight different PAX6 missense variants were identified in 17 individuals (15 families) with MAC, accounting for 4% (15/372) of our cohort. Seven altered the paired domain (p.[Arg26Gln]x1, p.[Gly36Val]x1, p.[Arg38Trp]x2, p.[Arg38Gln]x1, p.[Gly51Arg]x2, p.[Ser54Arg]x2, p.[Asn124Lys]x5) and one the homeodomain (p.[Asn260Tyr]x1). p.Ser54Arg and p.Asn124Lys were exclusively associated with severe bilateral microphthalmia. MAC-associated variants were predicted to alter but not ablate DNA interaction, consistent with the electrophoretic mobility shifts observed using mutant paired domains with well-characterized PAX6-binding sites. We found no strong evidence for novel PAX6-associated extraocular disease.ConclusionAltering the affinity and specificity of PAX6-binding genome-wide provides a plausible mechanism for the worse-than-null effects of MAC-associated missense variants.",

author = "Kathleen Williamson and Hall, {H. Nikki} and Liusaidh Owen and Benjamin Livesey and Isabel Hanson and G.G.W Adams and Simon Bodek and Patrick Calvas and Bruce Castle and Michael Clarke and Deng, {Alexander T} and Patrick Edery and Richard Fisher and Gabriele Gillessen-Kaesbach and Elise H{\'e}on and Jane Hurst and Dragana Josifova and Birgit Lorenz and Shane McKee and Francoise Meire and Moore, {Anthony T} and Michael Parker and Charlotte Reiff and Jay Self and Tobias, {Edward S} and Verheij, {Joke B. G. M.} and Marjolaine Willems and Denise Williams and {Van Heyningen}, Veronica and Marsh, {Joseph A.} and FitzPatrick, {David R.}",

year = "2019",

month = nov,

day = "8",

doi = "10.1038/s41436-019-0685-9",

language = "English",

journal = "Genetics in Medicine",

issn = "1098-3600",

publisher = "Lippincott Williams and Wilkins",

}

Williamson, K , Hall, HN, Owen, L, Livesey, B, Hanson, I, Adams, GGW, Bodek, S, Calvas, P, Castle, B, Clarke, M, Deng, AT, Edery, P, Fisher, R, Gillessen-Kaesbach, G, Héon, E, Hurst, J, Josifova, D, Lorenz, B, McKee, S, Meire, F, Moore, AT, Parker, M, Reiff, C, Self, J, Tobias, ES, Verheij, JBGM, Willems, M, Williams, D, Van Heyningen, V, Marsh, JA & FitzPatrick, DR 2019, 'Recurrent heterozygous PAX6 missense variants cause severe bilateral microphthalmia via predictable effects on DNA-protein interaction', Genetics in Medicine. https://doi.org/10.1038/s41436-019-0685-9

TY - JOUR

T1 - Recurrent heterozygous PAX6 missense variants cause severe bilateral microphthalmia via predictable effects on DNA-protein interaction

AU - Williamson, Kathleen

AU - Hall, H. Nikki

AU - Owen, Liusaidh

AU - Livesey, Benjamin

AU - Hanson, Isabel

AU - Adams, G.G.W

AU - Bodek, Simon

AU - Calvas, Patrick

AU - Castle, Bruce

AU - Clarke, Michael

AU - Deng, Alexander T

AU - Edery, Patrick

AU - Fisher, Richard

AU - Gillessen-Kaesbach, Gabriele

AU - Héon, Elise

AU - Hurst, Jane

AU - Josifova, Dragana

AU - Lorenz, Birgit

AU - McKee, Shane

AU - Meire, Francoise

AU - Moore, Anthony T

AU - Parker, Michael

AU - Reiff, Charlotte

AU - Self, Jay

AU - Tobias, Edward S

AU - Verheij, Joke B. G. M.

AU - Willems, Marjolaine

AU - Williams, Denise

AU - Van Heyningen, Veronica

AU - Marsh, Joseph A.

AU - FitzPatrick, David R.

PY - 2019/11/8

Y1 - 2019/11/8

N2 - PurposeMost classical aniridia is caused by PAX6 haploinsufficiency. PAX6 missense variants can be hypomorphic or mimic haploinsufficiency. We hypothesized that missense variants also cause previously undescribed disease by altering the affinity and/or specificity of PAX6 genomic interactions.MethodsWe screened PAX6 in 372 individuals with bilateral microphthalmia, anophthalmia, or coloboma (MAC) from the Medical Research Council Human Genetics Unit eye malformation cohort (HGUeye) and reviewed data from the Deciphering Developmental Disorders study. We performed cluster analysis on PAX6-associated ocular phenotypes by variant type and molecular modeling of the structural impact of 86 different PAX6 causative missense variants.ResultsEight different PAX6 missense variants were identified in 17 individuals (15 families) with MAC, accounting for 4% (15/372) of our cohort. Seven altered the paired domain (p.[Arg26Gln]x1, p.[Gly36Val]x1, p.[Arg38Trp]x2, p.[Arg38Gln]x1, p.[Gly51Arg]x2, p.[Ser54Arg]x2, p.[Asn124Lys]x5) and one the homeodomain (p.[Asn260Tyr]x1). p.Ser54Arg and p.Asn124Lys were exclusively associated with severe bilateral microphthalmia. MAC-associated variants were predicted to alter but not ablate DNA interaction, consistent with the electrophoretic mobility shifts observed using mutant paired domains with well-characterized PAX6-binding sites. We found no strong evidence for novel PAX6-associated extraocular disease.ConclusionAltering the affinity and specificity of PAX6-binding genome-wide provides a plausible mechanism for the worse-than-null effects of MAC-associated missense variants.

AB - PurposeMost classical aniridia is caused by PAX6 haploinsufficiency. PAX6 missense variants can be hypomorphic or mimic haploinsufficiency. We hypothesized that missense variants also cause previously undescribed disease by altering the affinity and/or specificity of PAX6 genomic interactions.MethodsWe screened PAX6 in 372 individuals with bilateral microphthalmia, anophthalmia, or coloboma (MAC) from the Medical Research Council Human Genetics Unit eye malformation cohort (HGUeye) and reviewed data from the Deciphering Developmental Disorders study. We performed cluster analysis on PAX6-associated ocular phenotypes by variant type and molecular modeling of the structural impact of 86 different PAX6 causative missense variants.ResultsEight different PAX6 missense variants were identified in 17 individuals (15 families) with MAC, accounting for 4% (15/372) of our cohort. Seven altered the paired domain (p.[Arg26Gln]x1, p.[Gly36Val]x1, p.[Arg38Trp]x2, p.[Arg38Gln]x1, p.[Gly51Arg]x2, p.[Ser54Arg]x2, p.[Asn124Lys]x5) and one the homeodomain (p.[Asn260Tyr]x1). p.Ser54Arg and p.Asn124Lys were exclusively associated with severe bilateral microphthalmia. MAC-associated variants were predicted to alter but not ablate DNA interaction, consistent with the electrophoretic mobility shifts observed using mutant paired domains with well-characterized PAX6-binding sites. We found no strong evidence for novel PAX6-associated extraocular disease.ConclusionAltering the affinity and specificity of PAX6-binding genome-wide provides a plausible mechanism for the worse-than-null effects of MAC-associated missense variants.

U2 - 10.1038/s41436-019-0685-9

DO - 10.1038/s41436-019-0685-9

M3 - Article

SN - 1098-3600

JO - Genetics in Medicine

JF - Genetics in Medicine

ER -

Recurrent heterozygous PAX6 missense variants cause severe bilateral microphthalmia via predictable effects on DNA-protein interaction

Abstract

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